2mg/dl. Increase in serum creatinine did not have an impact if peak creatinine did not reach 1.2 mg/dl or more. Early renal protection strategies after hospitalization may improve the outcome PLX-4720 ic50 of patients with cirrhosis admitted with complications. Disclosures: Paul J. Thuluvath – Advisory Committees or Review Panels: Gilead, Abbvie;

Grant/Research Support: Vertex, Gilead, BMS, Isai, Salix, Abbvie; Speaking and Teaching: Gilead, Onyx, Abbvie The following people have nothing to disclose: Anantha Nuthalapati, Nicholas Schluterman, Deborah Greenberg, Anuj Khanna Acute kidney injury (AKI) occurs frequently in decompensated cirrhosis both in an ambulatory (Tsien et al, Gut 2013) and in a hospital setting (Garcia-Tsao et al, Hepatology 2008). Most AKI episodes are functional renal disorders, precipitated by an acute event such as infection that perturbs the hemodynamics. Because the background

abnormal hemodynamics and compromised renal circulation in decompensated cirrhosis can further deteriorate, it is possible that AKI can occur without any precipitant. Aim: to determine the prevalence of unprecipitated AKI (acute in serum creatinine (SCr) by >0.3mg/ dL (26.4μmol/L) in ≤48 hours or by 50% from baseline) (Wong et al, Gut, 2011) in a large cohort of ambulatory & hospitalized decompensated cirrhotic patients. Methods: Database containing 1115 stable decompensated cirrhotics with ascites and no other complications (early ascites or Gp A: n=434, diuretic responsive ascites or Gp B: n=451, refractory ascites or Gp C: n=230) from several randomized controlled http://www.selleckchem.com/products/pexidartinib-plx3397.html vaptan trials was assessed. Two SCr readings selleck ≤7 days apart taken at screening and at randomization into the vaptan studies were used to determine AKI prevalence. No precipitating event was reported between the 2 SCr readings. Results: AKI had a prevalence of 1.8% in the entire cohort. The prevalence of unprecipitated AKI increases with worsening ascites severity (Gp A: 4/434 or 0.9%; Gp B: 7/451 or 1.6%; Gp C: 9/230 or 3.9%; p=0.019). AKI patients

had a mean screening SCr of 89±24μmol/L (±SD), increased to 130±31μmol/L (p<0.001) at AKI diagnosis. All patients except one had stage 1 AKI defined as in SCr by ≥26.4μmol/L or by 1.5-1.9X from screening. One patient had stage 2 AKI (2.0-2.9X in SCr from screening). Within a 7-day period, the AKI in 3 stage 1 patients progressed, two to stage 2, and 1 to stage 3 (>3.0 X in SCr from screening). There was no significant difference in terms of age, gender, liver cirrhosis etiology, history of diabetes or systemic hypertension, screening mean arterial pressure, heart rate, blood work or Child-Pugh and MELD scores, between those who developed AKI versus those who did not. However, there was a significant negative correlation between the screening serum Na and SCr (p=0.0008). Summary: AKI, unprecipitated by any acute event, still occurs in 1.